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Publication : Fate of retinoic acid-activated embryonic cell lineages.

First Author  Dollé P Year  2010
Journal  Dev Dyn Volume  239
Issue  12 Pages  3260-74
PubMed ID  21046629 Mgi Jnum  J:166703
Mgi Id  MGI:4849333 Doi  10.1002/dvdy.22479
Citation  Dolle P, et al. (2010) Fate of retinoic acid-activated embryonic cell lineages. Dev Dyn 239(12):3260-74
abstractText  Retinoic acid (RA), a vitamin A derivative, is synthesized by specific cell populations and acts as a diffusible embryonic signal activating ligand-inducible transcription factors, the RA receptors (RARs). RA-activatable transgenic systems have revealed many discrete, transient sites of RA action during development. However, there has been no attempt to permanently label the RA-activated cell lineages during mouse ontogenesis. We describe the characterization of a RA-activatable Cre transgene, which through crosses with a conditional reporter strain (the ROSA26R lacZ reporter), leads to a stable labeling of the cell populations experiencing RA signaling during embryogenesis. RA response-element (RARE)-driven Cre activity mimics at early stages the known activity of the corresponding RARE-lacZ transgene (Rossant et al.,1991). Stable labeling of the Cre-excised cell populations allows to trace the distribution of the RA-activated cell lineages at later stages. These are described in relationship with current models of RA activity in various developmental systems, including the embryonic caudal region, limb buds, hindbrain, sensory organs, and heart.
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